Harrison H H, Gordon E D, Nichols W C, Benson M D
Dept. of Pathology, University of Chicago Pritzker School of Medicine, IL 60637.
Am J Med Genet. 1991 Jun 15;39(4):442-52. doi: 10.1002/ajmg.1320390415.
We report identification, biochemical, clinical, and genetic studies of an apparently benign, electrophoretic variant of serum prealbumin (PALB, transthyretin, TTR) in a North American kindred of Swedish ancestry. The variant polypeptide stems from a C to T point mutation in exon 4 which results in methionine instead of threonine at position 119 of the mature molecule. It was discovered incidentally in a girl with classic alpha-1-anti-trypsin (A1AT) deficiency and her father during diagnostic A1AT phenotyping by ISO-DALT high-resolution two-dimensional electrophoresis (2DE). Twelve relatives in the four-generation paternal kindred, including five individuals who were heterozygous for the variant prealbumin, were studied. In each of these five heterozygotes, the variant allele product was equimolar and isoelectric with the normal protein, yet migrated with an apparently lower mass in the SDS-PAGE dimension. The inheritance pattern was consistent with autosomal dominant transmission. Histories and physical examinations showed no evidence of amyloidosis, as has been observed with other variants of prealbumin. Mean values of serum prealbumin and retinol binding protein levels were higher in the carriers as compared to the normal relatives in the family, but the difference was not statistically significant. Thyroid hormone levels and distribution of thyroxine and triiodothyronine among binding proteins in serum were within reference limits. Four members of the lineage had dominant, scalp-restricted keratinaceous cysts, yet only three of these four individuals had the variant. We counseled the family that this is likely a benign variant with regard to amyloidosis-related morbidity or shortened life span, although senile effects cannot be entirely ruled out. The provisional designation assigned to this allele is PALBCHICAGO. The substitution of methionine at position 119, as predicted by the DNA sequence, was confirmed by amino acid sequencing of CNBr and tryptic peptides. This substitution occurs at a CpG dinucleotide that may be a point mutational "hot spot," as has been postulated for the methionine-30 and isoleucine-122 PALB variants. The apparently lower mass of the variant probably results from a more compact conformation in SDS. With the exception of histidine-58, a charge substitution, all other amyloidosis-related prealbumin variant polypeptides had normal mobility in the ISO-DALT 2DE system.
我们报告了对北美一个具有瑞典血统的家族中血清前白蛋白(PALB,转甲状腺素蛋白,TTR)一种明显良性的电泳变体进行的鉴定、生化、临床和遗传学研究。该变体多肽源于外显子4中的一个C到T点突变,导致成熟分子第119位的苏氨酸被甲硫氨酸取代。它是在一名患有经典α-1-抗胰蛋白酶(A1AT)缺乏症的女孩及其父亲通过ISO-DALT高分辨率二维电泳(2DE)进行A1AT表型诊断时偶然发现的。对这个四代父系家族中的12名亲属进行了研究,其中包括5名该变体前白蛋白杂合子个体。在这5名杂合子中的每一个中,变体等位基因产物与正常蛋白质等摩尔且等电,但在SDS-PAGE维度中迁移时质量明显较低。遗传模式符合常染色体显性遗传。病史和体格检查未发现淀粉样变性的证据,这与其他前白蛋白变体的情况一致。与家族中的正常亲属相比,携带者的血清前白蛋白和视黄醇结合蛋白水平平均值较高,但差异无统计学意义。甲状腺激素水平以及血清中甲状腺素和三碘甲状腺原氨酸在结合蛋白中的分布均在参考范围内。该家族谱系中有4名成员患有显性的、局限于头皮的角质囊肿,但这4人中只有3人有该变体。我们告知该家族,就淀粉样变性相关的发病率或缩短的寿命而言,这可能是一种良性变体,尽管不能完全排除衰老的影响。赋予该等位基因的临时名称是PALBCHICAGO。如DNA序列所预测的,第119位甲硫氨酸的取代通过对溴化氰和胰蛋白酶肽段的氨基酸测序得到证实。这种取代发生在一个CpG二核苷酸处,该二核苷酸可能是一个点突变“热点”,正如对甲硫氨酸-30和异亮氨酸-122 PALB变体所假设的那样。变体明显较低的质量可能是由于在SDS中构象更紧密。除了电荷取代的组氨酸-58外,所有其他与淀粉样变性相关的前白蛋白变体多肽在ISO-DALT 2DE系统中迁移率正常。
